Haploinsufficiency of TCF4 causes syndromal mental retardation with intermittent hyperventilation (Pitt-Hopkins syndrome).

Pitt-Hopkins syndrome is a rarely reported syndrome of so-far-unknown etiology characterized by mental retardation, wide mouth, and intermittent hyperventilation. By molecular karyotyping with GeneChip Human Mapping 100K SNP arrays, we detected a 1.2-Mb deletion on 18q21.2 in one patient. Sequencing of the TCF4 transcription factor gene, which is contained in the deletion region, in 30 patients with significant phenotypic overlap revealed heterozygous stop, splice, and missense mutations in five further patients with severe mental retardation and remarkable facial resemblance. Thus, we establish the Pitt-Hopkins syndrome as a distinct but probably heterogeneous entity caused by autosomal dominant de novo mutations in TCF4. Because of its phenotypic overlap, Pitt-Hopkins syndrome evolves as an important differential diagnosis to Angelman and Rett syndromes. Both null and missense mutations impaired the interaction of TCF4 with ASCL1 from the PHOX-RET pathway in transactivating an E box-containing reporter construct; therefore, hyperventilation and Hirschsprung disease in patients with Pitt-Hopkins syndrome might be explained by altered development of noradrenergic derivatives.

[1]  Meredith Wilson,et al.  ZFHX1B mutations in patients with Mowat‐Wilson syndrome , 2007, Human mutation.

[2]  A Chakravarti,et al.  Hirschsprung disease, associated syndromes and genetics: a review , 2001, Journal of Medical Genetics.

[3]  E. Berry-Kravis,et al.  Congenital central hypoventilation syndrome: PHOX2B mutations and phenotype. , 2006, American journal of respiratory and critical care medicine.

[4]  R. Pfundt,et al.  A new chromosome 17q21.31 microdeletion syndrome associated with a common inversion polymorphism , 2006, Nature Genetics.

[5]  Andrew J Sharp,et al.  Discovery of previously unidentified genomic disorders from the duplication architecture of the human genome , 2006, Nature Genetics.

[6]  Andrew J Lees,et al.  Microdeletion encompassing MAPT at chromosome 17q21.3 is associated with developmental delay and learning disability , 2006, Nature Genetics.

[7]  R. Hennekam,et al.  Peters Plus syndrome is caused by mutations in B3GALTL, a putative glycosyltransferase. , 2006, American journal of human genetics.

[8]  L. Valanne,et al.  Pitt–Hopkins syndrome in two patients and further definition of the phenotype , 2006, Clinical dysmorphology.

[9]  S. Romana,et al.  Molecular karyotyping in human constitutional cytogenetics. , 2005, European journal of medical genetics.

[10]  I. Krantz,et al.  Clinical and mutational spectrum of Mowat-Wilson syndrome. , 2005, European journal of medical genetics.

[11]  Bart De Moor,et al.  Molecular Karyotyping: Array CGH Quality Criteria for Constitutional Genetic Diagnosis , 2005, The journal of histochemistry and cytochemistry : official journal of the Histochemistry Society.

[12]  F. Rüschendorf,et al.  Molecular karyotyping using an SNP array for genomewide genotyping , 2004, Journal of Medical Genetics.

[13]  Han G Brunner,et al.  Mutations in a new member of the chromodomain gene family cause CHARGE syndrome , 2004, Nature Genetics.

[14]  Arnold Munnich,et al.  Noradrenergic neuronal development is impaired by mutation of the proneural HASH-1 gene in congenital central hypoventilation syndrome (Ondine's curse). , 2003, Human molecular genetics.

[15]  M. Sigvardsson,et al.  The pTα promoter and enhancer are direct targets for transactivation by E box‐binding proteins , 2002 .

[16]  J. Gallego,et al.  MASH-1/RET pathway involvement in development of brain stem control of respiratory frequency in newborn mice. , 2001, Physiological genomics.

[17]  F. Torricelli,et al.  Possible case of Pitt-Hopkins syndrome in sibs. , 2001, American journal of medical genetics.

[18]  N. Nomura,et al.  Mutations in SIP1, encoding Smad interacting protein-1, cause a form of Hirschsprung disease , 2001, Nature Genetics.

[19]  T. Grundström,et al.  The basic helix‐loop‐helix transcription factor E2–2 is involved in T lymphocyte development , 2000, European journal of immunology.

[20]  H. Axelson,et al.  HASH-1 and E2-2 are expressed in human neuroblastoma cells and form a functional complex. , 2000, Biochemical and biophysical research communications.

[21]  G. Annéren,et al.  Monosomy 18q syndrome and atypical Rett syndrome in a girl with an interstitial deletion (18)(q21.1q22.3). , 1999, American journal of medical genetics.

[22]  S. K. Ray,et al.  A Splice Variant of E2–2 Basic Helix-Loop-Helix Protein Represses the Brain-specific Fibroblast Growth Factor 1 Promoter through the Binding to an Imperfect E-box* , 1998, The Journal of Biological Chemistry.

[23]  R. Hennekam,et al.  Mental retardation, "coarse" face, and hyperbreathing: confirmation of the Pitt-Hopkins syndrome. , 1998, American journal of medical genetics.

[24]  H. Weintraub,et al.  B-lymphocyte development is regulated by the combined dosage of three basic helix-loop-helix genes, E2A, E2-2, and HEB , 1996, Molecular and cellular biology.

[25]  H. Singh Mental retardation, macrostomia and hyperpnoea syndrome , 1993, Journal of paediatrics and child health.

[26]  T. Grundström,et al.  Helix-loop-helix transcriptional activators bind to a sequence in glucocorticoid response elements of retrovirus enhancers , 1991, Journal of virology.

[27]  D. Pitt,et al.  A Syndrome of Mental Retardation, Wide Mouth and Intermittent Overbreathing , 1978, Australian paediatric journal.